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A novel HIV-1 antiviral high throughput screening approach for the discovery of HIV-1 inhibitors.

机译:用于发现HIV-1抑制剂的新颖HIV-1抗病毒高通量筛选方法。

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Antiviral high throughput screens remain a viable option for identifying novel target inhibitors. However, few antiviral screens have been reduced to practice on an industrial scale. In this study, we describe an HIV-1 dual reporter assay that allows for the simultaneous evaluation of the potential antiviral activities and cytotoxicities of compounds in a high throughput screen (HTS) format. We validate the assay with known HIV-1 inhibitors and show that the antiviral and cytotoxic activities of compounds are reproducibly measured under screening conditions. In addition, we show that the assay exhibits parameters (e.g., signal-to-background ratios and Z' coefficients) suitable for high throughout screening. In a pilot screen, we demonstrate that non-specific or cytotoxic compounds represent a significant fraction of the hits identified in an antiviral screen and that these false positives are identified and deprioritized by the HIV-1 dual reporter assay at the primary screening step. We propose that the HIV-1 dual reporter assay represents a novel approach to HIV-1 antiviral screening that allows for the effective execution of industrial scale HTS campaigns with significantly greater returns on resource investment when compared to previous methods.
机译:抗病毒高通量筛选仍然是鉴定新型靶标抑制剂的可行选择。然而,很少有抗病毒筛选被减少以工业规模实践。在这项研究中,我们描述了一种HIV-1双重报告基因检测方法,该方法可以同时评估高通量筛选(HTS)格式的化合物的潜在抗病毒活性和细胞毒性。我们用已知的HIV-1抑制剂验证了该检测方法的有效性,并显示了在筛选条件下可重复测量化合物的抗病毒和细胞毒性活性。另外,我们表明该测定法展示了适用于整个筛选的高参数(例如,信噪比和Z'系数)。在中试筛选中,我们证明了非特异性或细胞毒性化合物代表了在抗病毒筛选中鉴定出的命中物中的很大一部分,并且这些假阳性在最初的筛选步骤中通过HIV-1双重报告基因测定得到了鉴定和优先处理。我们建议,HIV-1双重报告基因检测代表了一种针对HIV-1抗病毒筛选的新方法,与以前的方法相比,该方法可有效执行工业规模的HTS活动,并在资源投资方面获得显着更高的回报。

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